Structural Basis for Targeting T:T Mismatch with Triaminotriazine-Acridine Conjugate Induces a U-Shaped Head-to-Head Four-Way Junction in CTG Repeat DNA

被引:31
作者
Chien, Ching-Ming [4 ]
Wu, Pei-Ching [4 ]
Satange, Roshan [1 ]
Chang, Cheng-Chun [5 ]
Lai, Zi-Lun [5 ]
Hagler, Lauren [3 ]
Zimmerman, Steven C. [3 ]
Hou, Ming-Hon [1 ,2 ]
机构
[1] Natl Chung Hsing Univ, PhD Program Med Biotechnol, Inst Genom & Bioinformat, Taichung 402, Taiwan
[2] Natl Chung Hsing Univ, Dept Life Sci, Taichung 402, Taiwan
[3] Univ Illinois, Dept Chem, Urbana, IL 61801 USA
[4] Natl Chung Hsing Univ, Inst Genom & Bioinformat, Taichung 402, Taiwan
[5] Natl Chung Hsing Univ, Grad Inst Biomed Engn, Taichung 402, Taiwan
基金
美国国家卫生研究院;
关键词
MYOTONIC-DYSTROPHY; TRINUCLEOTIDE REPEATS; CRYSTAL-STRUCTURE; LIGAND; RECOGNITION; MECHANISMS; REPAIR;
D O I
10.1021/jacs.0c03591
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
The potent DNA-binding compound triaminotriazine-acridine conjugate (Z1) functions by targeting T:T mismatches in CTG trinucleotide repeats that are responsible for causing neurological diseases such as myotonic dystrophy type 1, but its binding mechanism remains unclear. We solved a crystal structure of Z1 in a complex with DNA containing three consecutive CTG repeats with three T:T mismatches. Crystallographic studies revealed that direct intercalation of two Z1 molecules at both ends of the CTG repeat induces thymine base flipping and DNA backbone deformation to form a four-way junction. The core of the complex unexpectedly adopts a U-shaped head-to-head topology to form a crossover of each chain at the junction site. The crossover junction is held together by two stacked G:C pairs at the central core that rotate with respect to each other in an X-shape to form two nonplanar minor-groove-aligned G center dot C center dot G center dot C tetrads. Two stacked G:C pairs on both sides of the center core are involved in the formation of pseudo-continuous duplex DNA. Four metal-mediated base pairs are observed between the N7 atoms of G and Co-II, an interaction that strongly preserves the central junction site. Beyond revealing a new type of ligand-induced, four-way junction, these observations enhance our understanding of the specific supramolecular chemistry of Z1 that is essential for the formation of a noncanonical DNA superstructure. The structural features described here serve as a foundation for the design of new sequence-specific ligands targeting mismatches in the repeat-associated structures.
引用
收藏
页码:11165 / 11172
页数:8
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